Quest for the right Drug
רבלימיד 20 מ"ג REVLIMID 20 MG (LENALIDOMIDE)
תרופה במרשם
תרופה בסל
נרקוטיקה
ציטוטוקסיקה
צורת מתן:
פומי : PER OS
צורת מינון:
קפסולה קשיחה : CAPSULE, HARD
עלון לרופא
מינוניםPosology התוויות
Indications תופעות לוואי
Adverse reactions התוויות נגד
Contraindications אינטראקציות
Interactions מינון יתר
Overdose הריון/הנקה
Pregnancy & Lactation אוכלוסיות מיוחדות
Special populations תכונות פרמקולוגיות
Pharmacological properties מידע רוקחי
Pharmaceutical particulars אזהרת שימוש
Special Warning עלון לרופא
Physicians Leaflet
Adverse reactions : תופעות לוואי
4.8 Undesirable effects Summary of the safety profile Newly diagnosed multiple myeloma: patients who have undergone ASCT treated with REVLIMID maintenance A conservative approach was applied to determine the adverse reactions from CALGB 100104. The adverse reactions described in Table 1 included events reported post-HDM/ASCT as well as events from the maintenance treatment period. A second analysis that identified events that occurred after the start of maintenance treatment suggests that the frequencies described in Table 1 may be higher than actually observed during the maintenance treatment period. In IFM 2005-02, the adverse reactions were from the maintenance treatment period only. The serious adverse reactions observed more frequently (≥5%) with REVLIMID maintenance than placebo were: • Pneumonia (10.6%; combined term) from IFM 2005-02 • Lung infection (9.4% [9.4% after the start of maintenance treatment]) from CALGB 100104 In the IFM 2005-02 study, the adverse reactions observed more frequently with REVLIMID maintenance than placebo were neutropenia (60.8%), bronchitis (47.4%), diarrhoea (38.9%), nasopharyngitis (34.8%), muscle spasms (33.4%), leucopenia (31.7%), asthenia (29.7%), cough (27.3%), thrombocytopenia (23.5%), gastroenteritis (22.5%) and pyrexia (20.5%). In the CALGB 100104 study, the adverse reactions observed more frequently with REVLIMID maintenance than placebo were neutropenia (79.0% [71.9% after the start of maintenance treatment]), thrombocytopenia (72.3% [61.6%]), diarrhoea (54.5% [46.4%]), rash (31.7% [25.0%]), upper respiratory tract infection (26.8% [26.8%]), fatigue (22.8% [17.9%]), leucopenia (22.8% [18.8%]) and anaemia (21.0% [13.8%]). Newly diagnosed multiple myeloma patients receiving REVLIMID in combination with bortezomib and dexamethasone In the SWOG S0777 study, the serious adverse reactions observed more frequently (≥ 5%) with REVLIMID in combination with intravenous bortezomib and dexamethasone than with REVLIMID in combination with dexamethasone were: • Hypotension (6.5%), lung infection (5.7%), dehydration (5.0%) The adverse reactions observed more frequently with REVLIMID in combination with bortezomib and dexamethasone than with REVLIMID in combination with dexamethasone were: Fatigue (73.7%), peripheral neuropathy (71.8%), thrombocytopenia (57.6%), constipation (56.1%), hypocalcaemia (50.0%). The most frequent adverse events with the Revlimid, bortezomib and dexamethasone combination across the 3 studies were in the System Organ Classes of Nervous System Disorders, Blood and Lymphatic System Disorders and Gastrointestinal Disorders. Compared with Revlimid and dexamethasone, the combination of Revlimid, bortezomib and dexamethasone was associated with increased incidences of treatment-emergent serious adverse events (40.1% RVd vs. 28.5% Rd) and discontinuations due to treatment emergent AEs (22.9% RVd vs. 9.4% Rd). Increases in the incidence of Grade 3/ 4 adverse events in the RVd arm versus the Rd arm were most notable for peripheral sensory and motor neuropathy, thrombocytopenia, hypotension, diarrhoea, syncope, hypokalaemia and dehydration. Newly diagnosed multiple myeloma: patients who are not eligible for transplant treated with REVLIMID in combination with low dose dexamethasone The serious adverse reactions observed more frequently (≥5%) with REVLIMID in combination with low dose dexamethasone (Rd and Rd18) than with melphalan, prednisone and thalidomide (MPT) were: • Pneumonia (9.8%) • Renal failure (including acute) (6.3%) The adverse reactions observed more frequently with Rd or Rd18 than MPT were: diarrhoea (45.5%), fatigue (32.8%), back pain (32.0%), asthenia (28.2%), insomnia (27.6%), rash (24.3%), decreased appetite (23.1%), cough (22.7%), pyrexia (21.4%), and muscle spasms (20.5%). Newly diagnosed multiple myeloma: patients who are not eligible for transplant treated with REVLIMID in combination with melphalan and prednisone The serious adverse reactions observed more frequently (≥5%) with melphalan, prednisone and REVLIMID followed by REVLIMID maintenance (MPR+R) or melphalan, prednisone and REVLIMID followed by placebo (MPR+p) than melphalan, prednisone and placebo followed by placebo (MPp+p) were: • Febrile neutropenia (6.0%) • Anaemia (5.3%) The adverse reactions observed more frequently with MPR+R or MPR+p than MPp+p were: neutropenia (83.3%), anaemia (70.7%), thrombocytopenia (70.0%), leucopenia (38.8%), constipation (34.0%), diarrhoea (33.3%), rash (28.9%), pyrexia (27.0%), peripheral oedema (25.0%), cough (24.0%), decreased appetite (23.7%), and asthenia (22.0%). Multiple myeloma: patients with at least one prior therapy In two phase 3 placebo-controlled studies, 353 patients with multiple myeloma were exposed to the REVLIMID/dexamethasone combination and 351 to the placebo/dexamethasone combination. The most serious adverse reactions observed more frequently in REVLIMID/dexamethasone than placebo/dexamethasone combination were: • Venous thromboembolism (deep vein thrombosis, pulmonary embolism) (see section 4.4) • Grade 4 neutropenia (see section 4.4) The observed adverse reactions which occurred more frequently with REVLIMID and dexamethasone than placebo and dexamethasone in pooled multiple myeloma clinical trials (MM-009 and MM-010) were fatigue (43.9%), neutropenia (42.2%), constipation (40.5%), diarrhoea (38.5%), muscle cramp (33.4%), anaemia (31.4%), thrombocytopenia (21.5%), and rash (21.2%). Myelodysplastic syndromes The overall safety profile of REVLIMID in patients with myelodysplastic syndromes is based on data from a total of 286 patients from one phase 2 study and one phase 3 study (see section 5.1). In the phase 2, all 148 patients were on REVLIMID treatment. In the phase 3 study, 69 patients were on REVLIMID 5 mg, 69 patients on REVLIMID 10 mg and 67 patients were on placebo during the double-blind phase of the study. Most adverse reactions tended to occur during the first 16 weeks of therapy with REVLIMID. Serious adverse reactions include: • Venous thromboembolism (deep vein thrombosis, pulmonary embolism) (see section 4.4) • Grade 3 or 4 neutropenia, febrile neutropenia and Grade 3 or 4 thrombocytopenia (see section 4.4). The most commonly observed adverse reactions which occurred more frequently in the REVLIMID groups compared to the control arm in the phase 3 study were neutropenia (76.8%), thrombocytopenia (46.4%), diarrhoea (34.8%), constipation (19.6%), nausea (19.6%), pruritus (25.4%), rash (18.1%), fatigue (18.1%) and muscle spasms (16.7%). Mantle cell lymphoma The overall safety profile of Revlimid in patients with mantle cell lymphoma is based on data from 254 patients from a phase 2 randomised, controlled study MCL-002 (see section 5.1). Additionally, adverse drug reactions from supportive study MCL-001 have been included in table 3. The serious adverse reactions observed more frequently in study MCL-002 (with a difference of at least 2 percentage points) in the REVLIMID arm compared with the control arm were: • Neutropenia (3.6%) • Pulmonary embolism (3.6%) • Diarrhoea (3.6%) The most frequently observed adverse reactions which occurred more frequently in the REVLIMID arm compared with the control arm in study MCL-002 were neutropenia (50.9%), anaemia (28.7%), diarrhoea (22.8%), fatigue (21.0%), constipation (17.4%), pyrexia (16.8%), and rash (including dermatitis allergic) (16.2%). In study MCL-002 there was overall an apparent increase in early (within 20 weeks) deaths. Patients with high tumour burden at baseline are at increased risk of early death, 16/81 (20%) early deaths in the REVLIMID arm and 2/28 (7%) early deaths in the control arm. Within 52 weeks corresponding figures were 32/81 (39.5%) and 6/28 (21%) (see section 5.1). During treatment cycle 1, 11/81 (14%) patients with high tumour burden were withdrawn from therapy in the REVLIMID arm vs. 1/28 (4%) in the control group. The main reason for treatment withdrawal for patients with high tumour burden during treatment cycle 1 in the REVLIMID arm was adverse events, 7/11 (64%). High tumour burden was defined as at least one lesion ≥5 cm in diameter or 3 lesions ≥3 cm. Follicular lymphoma The overall safety profile of REVLIMID in combination with rituximab in patients with previously treated follicular lymphoma is based on data from 294 patients from a Phase 3 randomised, controlled study NHL-007. Additionally, adverse drug reactions from supportive study NHL-008 have been included in Table 5. The serious adverse reactions observed most frequently (with a difference of at least 1 percentage point) in study NHL-007 in the REVLIMID/rituximab arm compared with the placebo/rituximab arm were: • Febrile neutropenia (2.7%) • Pulmonary embolism (2.7%) • Pneumonia (2.7%) In the NHL-007 study the adverse reactions observed more frequently in the REVLIMID/rituximab arm compared with the placebo/rituximab arm (with at least 2% higher frequency between arms) were neutropenia (58.2%), diarrhoea (30.8%), leucopenia (28.8%), constipation (21.9%), cough (21.9%) and fatigue (21.9%). Tabulated list of adverse reactions The adverse reactions observed in patients treated with Revlimid are listed below by system organ class and frequency. Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness. Frequencies are defined as: very common (≥ 1/10); common (≥ 1/100 to < 1/10); uncommon (≥ 1/1,000 to < 1/100); rare (≥ 1/10,000 to < 1/1,000); very rare (< 1/10,000), not known (cannot be estimated from the available data). Adverse reactions have been included under the appropriate category in the table below according to the highest frequency observed in any of the main clinical trials. Tabulated summary for monotherapy in MM The following table is derived from data gathered during NDMM studies in patients who have undergone ASCT treated with REVLIMID maintenance. The data were not adjusted according to the longer duration of treatment in the REVLIMID-containing arms continued until disease progression versus the placebo arms in the pivotal multiple myeloma studies (see section 5.1). Table 1. ADRs reported in clinical trials in patients with multiple myeloma treated with REVLIMID maintenance therapy System Organ Class/Preferred All ADRs/Frequency Grade 3-4 ADRs/Frequency Term Very Common Very Common Pneumonia◊,a, Upper respiratory Pneumonia◊,a, Neutropenic tract infection, Neutropenic infection infection, Bronchitis◊, Influenza◊, Gastroenteritis◊, Sinusitis, Common Infections and Infestations Nasopharyngitis, Rhinitis Sepsis◊,b, Bacteraemia, Lung infection◊, Lower respiratory tract Common infection bacterial, Bronchitis◊, Infection◊, Urinary tract Influenza◊, Gastroenteritis◊, ◊, infection *, Lower respiratory Herpes zoster◊, Infection◊ ◊ tract infection, Lung infection Neoplasms Benign, Malignant Common and Unspecified (incl cysts and Myelodysplastic syndrome◊,* polyps) Very Common Very Common Neutropenia^,◊, Febrile Neutropenia^,◊, Febrile ^,◊ neutropenia , neutropenia^,◊, Blood and Lymphatic System Thrombocytopenia^,◊, Anaemia, Thrombocytopenia^,◊, Anaemia, ◊ Disorders Leucopenia , Lymphopenia Leucopenia◊, Lymphopenia Common Pancytopenia◊ Metabolism and Nutrition Very Common Common Disorders Hypokalaemia Hypokalaemia, Dehydration Very Common Common Paraesthesia Headache Nervous System Disorders Common Peripheral neuropathyc Vascular Disorders Common Common System Organ Class/Preferred All ADRs/Frequency Grade 3-4 ADRs/Frequency Term Pulmonary embolism◊,* Deep vein thrombosis^,◊,d Very Common Common Cough Dyspnoea◊ Respiratory, Thoracic and Mediastinal Disorders Common Dyspnoea◊, Rhinorrhoea Very Common Common Diarrhoea, Constipation, Abdominal Diarrhoea, Vomiting, Nausea pain, Nausea Gastrointestinal Disorders Common Vomiting, Abdominal pain upper Very Common Common Hepatobiliary Disorders Abnormal liver function tests Abnormal liver function tests Skin and Subcutaneous Tissue Very Common Common Disorders Rash, Dry skin Rash, Pruritus Very Common Muscle spasms Musculoskeletal and Connective Tissue Disorders Common Myalgia, Musculoskeletal pain General Disorders and Very Common Common Administration Site Conditions Fatigue, Asthenia, Pyrexia Fatigue, Asthenia ◊ Adverse reactions reported as serious in clinical trials in patients with NDMM who had undergone ASCT * Applies to serious adverse drug reactions only ^ See section 4.8 description of selected adverse reactions a “Pneumonia” combined AE term includes the following PTs: Bronchopneumonia, Lobar pneumonia, Pneumocystis jiroveci pneumonia, Pneumonia, Pneumonia klebsiella, Pneumonia legionella, Pneumonia mycoplasmal, Pneumonia pneumococcal, Pneumonia streptococcal, Pneumonia viral, Lung disorder, Pneumonitis b “Sepsis” combined AE term includes the following PTs: Bacterial sepsis, Pneumococcal sepsis, Septic shock, Staphylococcal sepsis c “Peripheral neuropathy” combined AE term includes the following preferred terms (PTs): Neuropathy peripheral, Peripheral sensory neuropathy, Polyneuropathy d “Deep vein thrombosis” combined AE term includes the following PTs: Deep vein thrombosis, Thrombosis, Venous thrombosis Tabulated summary for combination therapy in MM The following table is derived from data gathered during the multiple myeloma studies with combination therapy. The data were not adjusted according to the longer duration of treatment in the REVLIMID-containing arms continued until disease progression versus the comparator arms in the pivotal multiple myeloma studies (see section 5.1). Table 2. ADRs reported in clinical studies in patients with multiple myeloma treated with REVLIMID in combination with bortezomib and dexamethasone, dexamethasone, or melphalan and prednisone System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Infections Very Common Common and Infestations Pneumonia◊,◊◊, Upper respiratory tract Pneumonia◊,◊◊, Bacterial, viral ◊ infection , Bacterial, viral and fungal and fungal infections infections (including opportunistic (including opportunistic infections)◊, Nasopharyngitis, Pharyngitis, infections)◊, Cellulitis◊, Bronchitis◊, Rhinitis Sepsis◊,◊◊, Lung infection◊◊, Common Bronchitis◊, Respiratory tract Sepsis◊,◊◊, Lung infection◊◊, Urinary tract infection◊◊, Urinary tract ◊◊ ◊ infection , Sinusitis infection◊◊, Enterocolitis infectious Neoplasms Uncommon Common ^,◊ Benign, Basal cell carcinoma , Acute myeloid leukaemia◊, ^,◊, Malignant and Squamous skin cancer * Myelodysplastic syndrome◊, Unspecified (incl Squamous cell carcinoma of cysts and polyps) skin^,◊,** Uncommon T-cell type acute leukaemia◊, Basal cell carcinoma^,◊, Tumour lysis syndrome Blood and Very Common Very Common ^,◊,◊◊ ^,◊,◊◊ Lymphatic Neutropenia , Thrombocytopenia , Neutropenia^,◊,◊◊, ◊ ^ System Disorders Anaemia , Haemorrhagic disorder , Thrombocytopenia^,◊,◊◊, Leucopenia, Lymphopenia Anaemia◊, Leucopenia, Lymphopenia Common Febrile neutropenia^,◊, Pancytopenia◊ Common Febrile neutropenia^,◊, Uncommon Pancytopenia◊, Haemolytic Haemolysis, Autoimmune haemolytic anaemia anaemia, Haemolytic anaemia Uncommon Hypercoagulation, Coagulopathy Immune System Uncommon Disorders Hypersensitivity^ Endocrine Common Disorders Hypothyroidism System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Metabolism and Very Common Common Nutrition Hypokalaemia◊,◊◊, Hyperglycaemia, Hypokalaemia◊,◊◊, Disorders Hypoglycaemia, Hypocalcaemia◊, Hyperglycaemia, Hyponatraemia◊, Dehydration◊◊, Decreased Hypocalcaemia◊, Diabetes appetite◊◊, Weight decreased mellitus◊, Hypophosphataemia, Common Hyponatraemia◊, Hypomagnesaemia, Hyperuricaemia, Hyperuricaemia, Gout, Hypercalcaemia+ Dehydration◊◊, Decreased appetite◊◊, Weight decreased Psychiatric Very Common Common Disorders Depression, Insomnia Depression, Insomnia Uncommon Loss of libido Nervous System Very Common Very Common Disorders Peripheral neuropathies◊◊, Paraesthesia, Peripheral neuropathies◊◊ Dizziness◊◊, Tremor, Dysgeusia, Headache Common Common Cerebrovascular accident◊, Ataxia, Balance impaired, Syncope◊◊, Dizziness◊◊, Syncope◊◊, Neuralgia, Dysaesthesia Neuralgia Uncommon Intracranial haemorrhage^,, Transient ischaemic attack, Cerebral ischemia Eye Disorders Very Common Common Cataracts, Blurred vision Cataract Common Uncommon Reduced visual acuity Blindness Ear and Common Labyrinth Deafness (Including Hypoacusis), Tinnitus Disorders Cardiac Common Common Disorders Atrial fibrillation◊,◊◊, Bradycardia Myocardial infarction Uncommon (including acute)^,◊, Atrial Arrhythmia, QT prolongation, Atrial flutter, fibrillation◊,◊◊, Congestive Ventricular extrasystoles cardiac failure◊, Tachycardia, Cardiac failure◊,◊◊, Myocardial ischemia◊ System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Vascular Very Common Very Common Disorders Venous thromboembolic events^, Venous thromboembolic predominantly deep vein thrombosis and events^, predominantly deep pulmonary embolism^,◊,◊◊, Hypotension◊◊ vein thrombosis and pulmonary embolism^,◊,◊◊ Common Common Hypertension, Ecchymosis^ Vasculitis, Hypotension◊◊, Hypertension Uncommon Ischemia, Peripheral ischemia, Intracranial venous sinus thrombosis Respiratory, Very Common Common Thoracic Dyspnoea◊,◊◊, Epistaxis^, Cough Respiratory distress◊, and Mediastinal Dyspnoea◊,◊◊, Pleuritic pain◊◊, Disorders Common Hypoxia◊◊ Dysphonia Gastrointestinal Very Common Common Disorders Diarrhoea◊,◊◊, Constipation◊, Abdominal Gastrointestinal pain◊◊, Nausea, Vomiting◊◊, Dyspepsia, Dry haemorrhage^,◊,◊◊, Small mouth, Stomatitis intestinal obstruction◊◊, Diarrhoea◊◊, Constipation◊, Common Abdominal pain◊◊, Nausea, Gastrointestinal haemorrhage (including Vomiting◊◊ rectal haemorrhage, haemorrhoidal haemorrhage, peptic ulcer haemorrhage and gingival bleeding)^,◊◊, Dysphagia Uncommon Colitis, Caecitis Hepatobiliary Very Common Common Disorders Alanine aminotransferase increased, Cholestasis◊, Hepatotoxicity, Aspartate aminotransferase increased Hepatocellular injury◊◊, Alanine aminotransferase Common increased, Abnormal liver Hepatocellular injury◊◊, Abnormal liver function tests◊ function tests◊, Hyperbilirubinaemia Uncommon Uncommon Hepatic failure^ Hepatic failure^ System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Skin and Very Common Common Subcutaneous Rashes◊◊, Pruritus Rashes◊◊ Tissue Disorders Common Uncommon Urticaria, Hyperhidrosis, Dry skin, Skin Drug rash with eosinophilia hyperpigmentation, Eczema, Erythema and systemic symptoms◊◊ Uncommon Drug rash with eosinophilia and systemic symptoms◊◊, Skin discolouration, Photosensitivity reaction Musculoskeletal Very Common Common and Connective Muscular weakness◊◊, Muscle spasms, Bone Muscular weakness◊◊, Bone Tissue Disorders pain◊, pain◊, Musculoskeletal and Musculoskeletal and connective tissue pain connective tissue pain and and discomfort (including back pain◊,◊◊), discomfort (including back Pain in extremity, Myalgia, Arthralgia◊ pain◊,◊◊) Common Uncommon Joint swelling Joint swelling Renal and Very Common Uncommon Urinary Renal tubular necrosis Disorders Renal failure (including acute)◊,◊◊ Common Haematuria^, Urinary retention, Urinary incontinence Uncommon Acquired Fanconi syndrome Reproductive Common System and Erectile dysfunction Breast Disorders General Very Common Very Common Disorders Fatigue◊,◊◊, Oedema (including peripheral Fatigue◊,◊◊ and oedema), Pyrexia◊,◊◊, Asthenia, Influenza Administration like illness syndrome (including pyrexia, Common Site Conditions cough, myalgia, musculoskeletal pain, Oedema peripheral, headache and rigors) Pyrexia◊,◊◊, Asthenia Common Chest pain◊,◊◊, Lethargy Investigations Very Common Blood alkaline phosphatase increased Common C-reactive protein increased System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Injury, Poisoning Common and Procedural Fall, Contusion^ Complications ◊◊Adverse reactions reported as serious in clinical trials in patients with NDMM who had received REVLIMID in combination with bortezomib and dexamethasone ^See section 4.8 description of selected adverse reactions ◊ Adverse reactions reported as serious in clinical trials in patients with multiple myeloma treated with REVLIMID in combination with dexamethasone, or with melphalan and prednisone + Applies to serious adverse drug reactions only * Squamous skin cancer was reported in clinical trials in previously treated myeloma patients with REVLIMID/dexamethasone compared to controls ** Squamous cell carcinoma of skin was reported in a clinical trial in newly diagnosed myeloma patients with REVLIMID/dexamethasone compared to controls Tabulated summary from monotherapy The following tables are derived from data gathered during the main studies in monotherapy for myelodysplastic syndromes and mantle cell lymphoma. Table 3. ADRs reported in clinical trials in patients with myelodysplastic syndromes treated with REVLIMID# System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Infections and Very Common Very Common Infestations Bacterial, viral and fungal infections Pneumonia◊ ◊ (including opportunistic infections) Common Bacterial, viral and fungal infections (including opportunistic infections)◊, Bronchitis Blood and Lymphatic Very Common Very Common System Disorders Thrombocytopenia^,◊, Neutropenia^,◊, Thrombocytopenia^,◊, Neutropenia^,◊, Leucopenia Leucopenia Common Febrile neutropenia^,◊ Endocrine Disorders Very Common Hypothyroidism Metabolism and Very Common Common Nutrition Disorders Decreased appetite Hyperglycaemia◊, Decreased appetite Common Iron overload, Weight decreased Psychiatric Disorders Common Altered mood◊,~ Nervous System Very Common Disorders Dizziness, Headache Common Paraesthesia System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Cardiac Disorders Common Acute myocardial infarction^,◊, Atrial fibrillation◊, Cardiac failure◊ Vascular Disorders Common Common Hypertension, Haematoma Venous thromboembolic events, predominantly deep vein thrombosis and pulmonary embolism^,◊ Respiratory, Thoracic Very Common and Mediastinal Epistaxis^ Disorders Gastrointestinal Very Common Common Disorders Diarrhoea◊, Abdominal pain (including Diarrhoea◊, Nausea, Toothache upper), Nausea, Vomiting, Constipation Common Dry mouth, Dyspepsia Hepatobiliary Common Common Disorders Abnormal liver function tests Abnormal liver function tests Skin and Subcutaneous Very Common Common Tissue Disorders Rashes, Dry Skin, Pruritus Rashes, Pruritus Musculoskeletal and Very Common Common Connective Tissue Muscle spasms, Musculoskeletal pain Back pain◊ Disorders (including back pain◊ and pain in extremity), Arthralgia, Myalgia Renal and Urinary Common Disorders Renal failure◊ General Disorders and Very Common Common Administration Site Fatigue, Peripheral oedema, Influenza Pyrexia Conditions like illness syndrome (including pyrexia, cough, pharyngitis, myalgia, musculoskeletal pain, headache) Injury, Poisoning and Common Procedural Fall Complications ^see section 4.8 description of selected adverse reactions ◊Adverse events reported as serious in myelodysplastic syndromes clinical trials ~Altered mood was reported as a common serious adverse event in the myelodysplastic syndromes phase 3 study; it was not reported as a Grade 3 or 4 adverse event Algorithm applied for inclusion in the SmPC: All ADRs captured by the phase 3 study algorithm are included in the EU SmPC. For these ADRs, an additional check of the frequency of the ADRs captured by the phase 2 study algorithm was undertaken and, if the frequency of the ADRs in the phase 2 study was higher than in the phase 3 study, the event was included in the EU SmPC at the frequency it occurred in the phase 2 study. # Algorithm applied for myelodysplastic syndromes: • Myelodysplastic syndromes phase 3 study (double-blind safety population, difference between REVLIMID 5/10mg and placebo by initial dosing regimen occurring in at least 2 subjects) o All treatment-emergent adverse events with ≥ 5% of subjects in REVLIMID and at least 2% difference in proportion between REVLIMID and placebo o All treatment-emergent Grade 3 or 4 adverse events in 1% of subjects in REVLIMID and at least 1% difference in proportion between REVLIMID and placebo o All treatment-emergent serious adverse events in 1% of subjects in REVLIMID and at least 1% difference in proportion between REVLIMID and placebo • Myelodysplastic syndromes phase 2 study o All treatment-emergent adverse events with ≥ 5% of REVLIMID treated subjects o All treatment-emergent Grade 3 or 4 adverse\events in 1% of REVLIMID treated subjects o All treatment-emergent serious adverse events in 1% of REVLIMID treated subjects Table 4. ADRs reported in clinical trials in patients with mantle cell lymphoma treated with REVLIMID System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Infections and Very Common Common Infestations Bacterial, viral and fungal Bacterial, viral and fungal infections infections (including opportunistic (including opportunistic infections)◊, infections)◊, Nasopharyngitis, Pneumonia◊ ◊ Pneumonia Common Sinusitis Neoplasms Common Common Benign, Tumour flare reaction Tumour flare reaction, Squamous skin Malignant and cancer^,◊, Basal cell carcinoma^,◊ Unspecified (incl cysts and polyps) Blood and Very Common Very Common Lymphatic Thrombocytopenia^, Neutropenia^,◊, Thrombocytopenia^, Neutropenia^,◊, System Leucopenia◊, Anaemia◊ Anaemia◊ Disorders Common Common Febrile neutropenia^,◊ Febrile neutropenia^,◊, Leucopenia◊ Metabolism Very Common Common and Nutrition Decreased appetite, Weight Dehydration◊, Hyponatraemia, Disorders decreased, Hypokalaemia Hypocalcaemia Common Dehydration◊ Psychiatric Common Disorders Insomnia Nervous Common Common System Dysgeuesia, Headache, neuropathy Peripheral sensory neuropathy, Disorders peripheral Lethargy Ear and Common Labyrinth Vertigo Disorders Cardiac Common Disorders Myocardial infarction (including acute)^,◊, Cardiac failure Vascular Common Common Disorders Hypotension◊ Deep vein thrombosis◊, pulmonary embolism^,◊, Hypotension◊ Respiratory, Very Common Common Thoracic and Dyspnoea◊ Dyspnoea◊ Mediastinal Disorders System Organ All ADRs/Frequency Grade 3−4 ADRs/Frequency Class / Preferred Term Gastrointestina Very Common Common l Disorders Diarrhoea◊, Nausea◊, Vomiting◊, Diarrhoea◊, Abdominal pain◊, Constipation Constipation Common Abdominal pain◊ Skin and Very Common Common Subcutaneous Rashes (including dermatitis Rashes Tissue allergic), Pruritus Disorders Common Night sweats, Dry skin Musculoskeleta Very Common Common l and Muscle spasms, Back pain Back pain, Muscular weakness◊, Connective Common Arthralgia, Pain in extremity Tissue Arthralgia, Pain in extremity, Disorders Muscular weakness◊ Renal and Common Urinary Renal failure◊ Disorders General Very Common Common Disorders and Fatigue, Asthenia◊, Peripheral Pyrexia◊, Asthenia◊, Fatigue Administration oedema, Influenza like illness Site Conditions syndrome (including pyrexia◊, cough) Common Chills ^see section 4.8 description of selected adverse reactions ◊Adverse events reported as serious in mantle cell lymphoma clinical trials Algorithm applied for mantle cell lymphoma: • Mantle cell lymphoma controlled phase 2 study o All treatment-emergent adverse events with ≥ 5% of subjects in REVLIMID arm and at least 2% difference in proportion between REVLIMID and control arm o All treatment-emergent Grade 3 or 4 adverse events in ≥1% of subjects in REVLIMID arm and at least 1.0% difference in proportion between REVLIMID and control arm o All Serious treatment-emergent adverse events in ≥1% of subjects in REVLIMID arm and at least 1.0% difference in proportion between REVLIMID and control arm • Mantle cell lymphoma single arm phase 2 study o All treatment-emergent adverse events with ≥ 5% of subjects o All Grade 3 or 4 treatment-emergent adverse events reported in 2 or more subjects o All Serious treatment-emergent adverse events reported in 2 or more subjects Tabulated summary for combination therapy in FL The following table is derived from data gathered during the main studies (NHL-007 and NHL-008) using REVLIMID in combination with rituximab for patients with follicular lymphoma. Table 5. ADRs reported in clinical trials in patients with follicular lymphoma treated with REVLIMID in combination with rituximab System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Infections and Very Common Common Infestations Upper respiratory tract infection Pneumonia◊, Sepsis◊, Lung infection, Common Bronchitis, Gastroenteritis, Sinusitis, Pneumonia◊, Influenza, Bronchitis, Urinary tract infection, Cellulitis◊ Sinusitis, Urinary tract infection Neoplasms Benign, Very Common Common Malignant and Tumour flare^ Basal cell carcinoma^,◊ Unspecified (incl cysts Common and polyps) Squamous Cell Carcinoma of Skin◊,^,+ Blood and Lymphatic Very Common Very Common System Disorders Neutropenia^,◊, Anaemia◊, Neutropenia^,◊ Thrombocytopenia^, Leucopenia** Common Lymphopenia*** Anaemia◊, Thrombocytopenia^, Febrile neutropenia◊, Pancytopenia, Leucopenia**, Lymphopenia*** Metabolism and Very Common Common Nutrition Disorders Decreased appetite, Hypokalaemia Dehydration, Hypercalcaemia◊, Common Hypokalaemia, Hypophosphataemia, Hypophosphataemia, Dehydration Hyperuricaemia Psychiatric Disorders Common Depression, Insomnia Nervous System Very Common Common Disorders Headache, Dizziness Syncope Common Peripheral sensory neuropathy, Dysgeusia Cardiac Disorders Uncommon Arrhythmia◊ Vascular Disorders Common Common Hypotension Pulmonary embolism^,◊, Hypotension Respiratory, Thoracic Very Common Common and Mediastinal Dyspnoea◊, Cough, Dyspnoea◊ Disorders Common Oropharyngeal pain, Dysphonia Gastrointestinal Very Common Common Disorders Abdominal pain◊, Diarrhoea, Abdominal pain◊, Diarrhoea, Constipation, Nausea, Vomiting, Constipation, Stomatitis Dyspepsia Common Upper abdominal pain, Stomatitis, Dry mouth Skin and Subcutaneous Very Common Common Tissue Disorders Rash*, Pruritus Rash*, Pruritus Common Dry skin, Night sweats, Erythema System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Musculoskeletal and Very Common Common Connective Tissue Muscle spasms, Back pain, Arthralgia Muscular weakness, Neck pain Disorders Common Pain in extremity, Muscular weakness, Musculoskeletal pain, Myalgia, Neck pain Renal and Urinary Common Disorders Acute kidney injury◊ General Disorders and Very Common Common Administration Site Pyrexia, Fatigue, Asthenia, Peripheral Fatigue, Asthenia Conditions oedema Common Malaise, Chills Investigations Very Common Alanine aminotransferase increased Common Weight decreased, Blood Bilirubin increased ^see section 4.8 description of selected adverse reactions Algorithm applied for follicular lymphoma: Controlled– Phase 3 trial: o NHL-007 ADRs- All treatment-emergent AEs with ≥ 5.0% of subjects in REVLIMID/rituximab arm and at least 2.0% higher frequency (%) in Len arm compared to control arm - (Safety population) o NHL-007 Gr 3/4 ADRs- All Grades 3 or Grade 4 treatment-emergent AEs with at least 1.0% subjects in REVLIMID/rituximab arm and at least 1.0% higher frequency in REVLIMID arm compared to control arm - (safety population) o NHL-007 Serious ADRs- All serious treatment-emergent AEs with at least 1.0% subjects in REVLIMID/rituximab arm and at least 1.0% higher frequency in REVLIMID/rituximab arm compared to control arm - (safety population) FL single arm - phase 3 trial: o NHL-008 ADRs- All treatment-emergent adverse events with ≥ 5.0% of subjects o NHL-008 Gr 3/4 ADRs- All Grade 3/4 treatment-emergent adverse events reported in ≥ 1.0% of subjects o NHL-008 Serious ADRs- All serious treatment-emergent adverse events reported in ≥ 1.0% of subjects ◊Adverse events reported as serious in follicular lymphoma clinical trials + Applies to serious adverse drug reactions only * Rash includes PT of rash and rash maculo-papular **Leucopenia includes PT leucopenia and white blood cell count decreased ***Lymphopenia includes PT lymphopenia and lymphocyte count decreased Tabulated summary of post-marketing adverse reactions In addition to the above adverse reactions identified from the pivotal clinical trials, the following table is derived from data gathered from post-marketing data. Table 6. ADRs reported in post-marketing use in patients treated with REVLIMID System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Infections and Not Known Not Known Infestations Viral infections, including herpes zoster and Viral infections, including herpes hepatitis B virus reactivation zoster and hepatitis B virus reactivation Neoplasms Benign, Rare Malignant and Tumour lysis syndrome Unspecified (incl cysts and polyps) System Organ Class / All ADRs/Frequency Grade 3−4 ADRs/Frequency Preferred Term Blood and Lymphatic Not Known System Disorders Acquired haemophilia Immune System Rare Rare Disorders Anaphylactic reaction^ Anaphylactic reaction^ Not Known Solid organ transplant rejection Endocrine Disorders Common Hyperthyroidism Respiratory, Thoracic Uncommon Rare and Mediastinal Pulmonary hypertension Pulmonary hypertension Disorders Not Known Interstitial pneumonitis Gastrointestinal Not Known Disorders Pancreatitis, Gastrointestinal perforation (including diverticular, intestinal and large intestine perforations)^ Hepatobiliary Disorders Not Known Not Known Acute hepatic failure^, Hepatitis toxic^, Acute hepatic failure^, Hepatitis Cytolytic hepatitis^, Cholestatic hepatitis^, toxic^ Mixed cytolytic/cholestatic hepatitis^ Skin and Subcutaneous Uncommon Tissue Disorders Angioedema Rare Stevens-Johnson Syndrome^, Toxic epidermal necrolysis^ Not Known Leukocytoclastic vasculitis, Drug Reaction with Eosinophilia and Systemic Symptoms^ ^see section 4.8 description of selected adverse reactions Description of selected adverse reactions Teratogenicity REVLIMID is structurally related to thalidomide. Thalidomide is a known human teratogenic active substance that causes severe life-threatening birth defects. In monkeys, REVLIMID induced malformations similar to those described with thalidomide (see sections 4.6 and 5.3). If REVLIMID is taken during pregnancy, a teratogenic effect of REVLIMID in humans is expected. Neutropenia and thrombocytopenia • Newly diagnosed multiple myeloma: patients who have undergone ASCT treated with REVLIMID maintenance REVLIMID maintenance after ASCT is associated with a higher frequency of Grade 4 neutropenia compared to placebo maintenance (32.1% vs 26.7% [16.1% vs 1.8% after the start of maintenance treatment] in CALGB 100104 and 16.4% vs 0.7% in IFM 2005-02, respectively). Treatment-emergent AEs of neutropenia leading to REVLIMID discontinuation were reported in 2.2% of patients in CALGB 100104 and 2.4% of patients in IFM 2005-02, respectively. Grade 4 febrile neutropenia was reported at similar frequencies in the REVLIMID maintenance arms compared to placebo maintenance arms in both studies (0.4% vs 0.5% [0.4% vs 0.5% after the start of maintenance treatment] in CALGB 100104 and 0.3% vs 0% in IFM 2005-02, respectively). REVLIMID maintenance after ASCT is associated with a higher frequency of Grade 3 or 4 thrombocytopenia compared to placebo maintenance (37.5% vs 30.3% [17.9% vs 4.1% after the start of maintenance treatment] in CALGB 100104 and 13.0% vs 2.9% in IFM 2005-02, respectively). • Newly diagnosed multiple myeloma patients who are not eligible for transplant receiving REVLIMID in combination with bortezomib and dexamethasone Grade 4 neutropenia was observed in the RVd arm to a lesser extent than in the Rd comparator arm (2.7% vs 5.9%) in the SWOG S0777 study. Grade 4 febrile neutropenia was reported at similar frequencies in the RVd arm compared to the Rd arm (0.0% vs 0.4%). Grade 3 or 4 thrombocytopenia was observed in the RVd arm to a greater extent than in the Rd comparator arm (17.2 % vs 9.4%). • Newly diagnosed multiple myeloma: patients who are not eligible for transplant treated with REVLIMID in combination with dexamethasone The combination of REVLIMID with dexamethasone in newly diagnosed multiple myeloma patients is associated with a lower frequency of Grade 4 neutropenia (8.5% in Rd and Rd18, compared with MPT (15%). Grade 4 febrile neutropenia was observed infrequently (0.6% in Rd and Rd18 compared with 0.7% in MPT). The combination of REVLIMID with dexamethasone in newly diagnosed multiple myeloma patients is associated with a lower frequency of Grade 3 and 4 thrombocytopenia (8.1% in Rd and Rd18) compared with MPT (11.1%). • Newly diagnosed multiple myeloma: patients who are not eligible for transplant treated with REVLIMID in combination with melphalan and prednisone The combination of REVLIMID with melphalan and prednisone in newly diagnosed multiple myeloma patients is associated with a higher frequency of Grade 4 neutropenia (34.1% in MPR+R/MPR+p) compared with MPp+p (7.8%). There was a higher frequency of Grade 4 febrile neutropenia observed (1.7% in MPR+R/MPR+p compared to 0.0% in MPp+p). The combination of REVLIMID with melphalan and prednisone in newly diagnosed multiple myeloma patients is associated with a higher frequency of Grade 3 and Grade 4 thrombocytopenia (40.4% in MPR+R/MPR+p) compared with MPp+p (13.7%). • Multiple myeloma: patients with at least one prior therapy The combination of REVLIMID with dexamethasone in multiple myeloma patients is associated with a higher incidence of Grade 4 neutropenia (5.1% in REVLIMID/dexamethasone-treated patients compared with 0.6% in placebo/dexamethasone-treated patients). Grade 4 febrile neutropenia episodes were observed infrequently (0.6% in REVLIMID/dexamethasone-treated patients compared to 0.0% in placebo/dexamethasone treated patients). The combination of REVLIMID with dexamethasone in multiple myeloma patients is associated with a higher incidence of Grade 3 and Grade 4 thrombocytopenia (9.9% and 1.4%, respectively, in REVLIMID/dexamethasone-treated patients compared to 2.3% and 0.0% in placebo/dexamethasone-treated patients). • Myelodysplastic syndromes patients In myelodysplastic syndromes patients, REVLIMID is associated with a higher incidence of Grade 3 or 4 neutropenia (74.6% in REVLIMID-treated patients compared with 14.9% in patients on placebo in the phase 3 study). Grade 3 or 4 febrile neutropenia episodes were observed in 2.2% of REVLIMID-treated patients compared with 0.0% in patients on placebo). REVLIMID is associated with a higher incidence of Grade 3 or 4 thrombocytopenia (37% in REVLIMID-treated patients compared with 1.5% in patients on placebo in the phase 3 study). • Mantle cell lymphoma patients In mantle cell lymphoma patients, REVLIMID is associated with a higher incidence of Grade 3 or 4 neutropenia (43.7% in REVLIMID-treated patients compared with 33.7% in patients in the control arm in the phase 2 study). Grade 3 or 4 febrile neutropenia episodes were observed in 6.0% of REVLIMID-treated patients compared with 2.4% in patients on control arm. • Follicular lymphoma patients The combination of REVLIMID with rituximab in follicular lymphoma is associated with a higher rate of grade 3 or grade 4 neutropenia (50.7% in REVLIMID/rituximab treated patients compared with 12.2% in placebo/rituximab treated patients). All grade 3 or 4 neutropenia were reversible through dose interruption, reduction and/or supportive care with growth factors. Additionally, febrile neutropenia was observed infrequently (2.7% in REVLIMID/rituximab treated patients compared with 0.7% in placebo/rituximab treated patients). REVLIMID in combination with rituximab is also associated with a higher incidence of grade 3 or 4 thrombocytopenia (1.4% in REVLIMID/rituximab treated patients compared to 0% in placebo/rituximab patients). Venous thromboembolism An increased risk of DVT and PE is associated with the use of the combination of REVLIMID with dexamethasone in patients with multiple myeloma, and to a lesser extent in patients treated with REVLIMID in combination with melphalan and prednisone or in patients with multiple myeloma, myelodysplastic syndromes and mantle cell lymphoma treated with REVLIMID monotherapy (see section 4.5). Concomitant administration of erythropoietic agents or previous history of DVT may also increase thrombotic risk in these patients. Myocardial infarction Myocardial infarction has been reported in patients receiving REVLIMID, particularly in those with known risk factors. Haemorrhagic disorders Haemorrhagic disorders are listed under several system organ classes: Blood and lymphatic system disorders; nervous system disorders (intracranial haemorrhage); respiratory, thoracic and mediastinal disorders (epistaxis); gastrointestinal disorders (gingival bleeding, haemorrhoidal haemorrhage, rectal haemorrhage); renal and urinary disorders (haematuria); injury, poisoning and procedural complications (contusion) and vascular disorders (ecchymosis). Allergic reactions and severe skin reactions Cases of allergic reactions including angioedema, anaphylactic reaction and severe cutaneous reactions including SJS, TEN and DRESS have been reported with the use of REVLIMID. A possible cross-reaction between REVLIMID and thalidomide has been reported in the literature. Patients with a history of severe rash associated with thalidomide treatment should not receive REVLIMID (see section 4.4). Second primary malignancies In clinical trials in previously treated myeloma patients with REVLIMID/dexamethasone compared to controls, mainly comprising of basal cell or squamous cell skin cancers. Acute myeloid leukaemia • Multiple myeloma Cases of AML have been observed in clinical trials of newly diagnosed multiple myeloma in patients taking REVLIMID treatment in combination with melphalan or immediately following HDM/ASCT (see section 4.4). This increase was not observed in clinical trials of newly diagnosed multiple myeloma in patients taking REVLIMID in combination with dexamethasone compared to thalidomide in combination with melphalan and prednisone. • Myelodysplastic syndromes Baseline variables including complex cytogenetics and TP53 mutation are associated with progression to AML in subjects who are transfusion dependent and have a Del (5q) abnormality (see section 4.4). The estimated 2- year cumulative risk of progression to AML were 13.8% in patients with an isolated Del (5q) abnormality compared to 17.3% for patients with Del (5q) and one additional cytogenetic abnormality and 38.6% in patients with a complex karyotype. In a post-hoc analysis of a clinical trial of REVLIMID in myelodysplastic syndromes, the estimated 2-year rate of progression to AML was 27.5 % in patients with IHC-p53 positivity and 3.6% in patients with IHC-p53 negativity (p=0.0038). In the patients with IHC-p53 positivity, a lower rate of progression to AML was observed amongst patients who achieved a transfusion independence (TI) response (11.1%) compared to a non- responder (34.8%). Hepatic disorders The following post-marketing adverse reactions have been reported (frequency unknown): acute hepatic failure and cholestasis (both potentially fatal), toxic hepatitis, cytolytic hepatitis, mixed cytolytic/cholestatic hepatitis. Rhabdomyolysis Rare cases of rhabdomyolysis have been observed, some of them when REVLIMID is administered with a statin. Thyroid disorders Cases of hypothyroidism and cases of hyperthyroidism have been reported (see section 4.4 Thyroid disorders). Tumour flare reaction and tumour lysis syndrome In study MCL-002, approximately 10% of REVLIMID-treated patients experienced TFR compared to 0% in the control arm. The majority of the events occurred in cycle 1, all were assessed as treatment-related, and the majority of the reports were grade 1 or 2. Patients with high MIPI at diagnosis or bulky disease (at least one lesion that is ≥ 7 cm in the longest diameter) at baseline may be at risk of TFR. In study MCL-002, TLS was reported for one patient in each of the two treatment arms. In the supportive study MCL-001, approximately 10% of subjects experienced TFR; all report were grade 1 or 2 in severity and all were assessed as treatment- related. The majority of the events occurred in cycle 1. There were no reports of TLS in study MCL-001 (see section 4.4). In study NHL-007, TFR was reported in 19/146 (13.0%) of patients in the REVLIMID/rituximab arm versus 1/148 (0.7%) patients in the placebo/rituximab arm. Most TFRs (18 out of 19) reported in the REVLIMID/rituximab arm occurred during first two cycles of treatment. One FL patient in the REVLIMID/rituximab arm experienced a Grade 3 TFR event versus no patients in the placebo/rituximab arm. In study NHL-008, 7/177 (4.0%) of FL patients experienced TFR; (3 reports were Grade 1 and 4 reports were Grade 2 severity); while 1 report was considered serious. In study NHL-007, TLS occurred in 2 FL patients (1.4%) in the REVLIMID/rituximab arm and no FL patients in the placebo/rituximab arm; neither patient had a Grade 3 or 4 event. TLS occurred in 1 FL patient (0.6%) in study NHL-008. This single event was identified as a serious, Grade 3 adverse reaction. For study NHL-007 no patients had to discontinue REVLIMID/rituximab therapy due to TFR or TLS. Gastrointestinal disorders Gastrointestinal perforations have been reported during treatment with REVLIMID. Gastrointestinal perforations may lead to septic complications and may be associated with fatal outcome. Reporting of suspected adverse reactions Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Any suspected adverse events should be reported to the Ministry of Health according to the National Regulation by using an online form https://sideeffects.health.gov.il and emailed to the Registration Holder’s Patient Safety Unit at: drugsafety@neopharmgroup.com
פרטי מסגרת הכללה בסל
א. התרופה האמורה תינתן לטיפול במקרים האלה: 1. מיאלומה נפוצה ובהתקיים אחד מאלה: א. חולה שטרם קיבל טיפול למחלתו ואינו מועמד להשתלת מח עצם.הטיפול יינתן בשילוב עם Dexamethasone או בשילוב עם Dexamethasone ו-Bortezomib.ב. מונותרפיה כטיפול אחזקה במאובחן חדש לאחר השתלת מח עצם.ג. חולה שמחלתו עמידה או נשנית לאחר מיצוי קו טיפול אחד שכלל אחד מהשניים - BORTEZOMIB או THALIDOMIDE, אלא אם כן לחולה הייתה הורית נגד לאחד מהטיפולים האמורים. על אף האמור בפסקה זו הטיפול בתכשיר ייפסק בחולה העונה על אחד מאלה: א. בחולה שמחלתו התקדמה לאחר שני מחזורי טיפול מלאים או ארבעה מחזורי טיפול חלקיים. ב. חולה שפיתח תופעות לוואי קשות לטיפול. הטיפול בתכשיר יינתן לחולה שטרם טופל ב-Lenalidomide למחלה זו. 2. תסמונת מיאלודיספלסטית ברמת חומרה low או intermediate-1 עם הפרעה ציטוגנטית מסוג deletion 5q. 3. בשילוב עם Rituximab, לטיפול בלימפומה פוליקולרית כקו טיפול מתקדם.ב. מתן התרופה האמורה ייעשה לפי מרשם של מומחה בהמטולוגיה.
מסגרת הכללה בסל
התוויות הכלולות במסגרת הסל
התוויה | תאריך הכללה | תחום קליני | Class Effect | מצב מחלה |
---|---|---|---|---|
בשילוב עם Rituximab, לטיפול בלימפומה פוליקולרית כקו טיפול מתקדם | 01/03/2021 | המטולוגיה | לימפומה פוליקולרית, Follicular lymphoma | |
מיאלומה נפוצה ובהתקיים אחד מאלה: א. חולה שטרם קיבל טיפול למחלתו ואינו מועמד להשתלת מח עצם. הטיפול יינתן בשילוב עם Dexamethasone או בשילוב עם Dexamethasone ו-Bortezomib. ב. כטיפול אחזקה במאובחן חדש לאחר השתלת מח עצם. | 16/01/2019 | המטולוגיה | מיאלומה נפוצה, Multiple myeloma | |
תסמונת מיאלודיספלסטית ברמת חומרה low או intermediate-1 עם הפרעה ציטוגנטית מסוג deletion 5q. | 10/01/2012 | המטולוגיה | MDS, Myelodysplastic syndrome | |
א. התרופה האמורה תינתן לטיפול במיאלומה נפוצה בחולה שמחלתו עמידה או נשנית לאחר מיצוי קו טיפול אחד שכלל אחד מהשניים – Bortezomib או Thalidomide, אלא אם לחולה הייתה הורית נגד לאחד מהטיפולים האמורים. ב. על אף האמור בפסקת משנה א הטיפול בתכשיר ייפסק: 1. בחולה שמחלתו התקדה לאחר שני מחזורי טיפול מלאים או ארבעה מחזורי טיפול חלקיים. 2. חולה שפיתח תופעות לוואי קשות לטיפול. ג. הטיפול בתכשיר יינתן לחולה שטרם טופל ב-Lenalidomide למחלה זו. | 23/01/2011 | המטולוגיה | מיאלומה נפוצה, Multiple myeloma | |
א. התרופה האמורה תינתן לטיפול במיאלומה נפוצה בחולה שמחלתו עמידה או נשנית לאחר לפחות שני קווי טיפול שכללו BORTEZOMIB ו-THALIDOMIDE, אלא אם לחולה הייתה הורית נגד לאחד מהטיפולים האמורים. ב. על אף האמור בפסקת משנה (א) הטיפול בתכשיר ייפסק: 1. בחולה שמחלתו התקדמה לאחר שני מחזורי טיפול מלאים או ארבעה מחזורי טיפול חלקיים. 2. חולה שפיתח תופעות לוואי קשות לטיפול. ג. הטיפול בתכשיר יינתן לחולה שטרם טופל ב-LENALIDOMIDE למחלה זו. | 03/01/2010 | המטולוגיה | מיאלומה נפוצה, Multiple myeloma |
שימוש לפי פנקס קופ''ח כללית 1994
לא צוין
תאריך הכללה מקורי בסל
03/01/2010
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